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. 2003 Jun;11(6):1647-59.
doi: 10.1016/s1097-2765(03)00235-1.

V体育官网 - Structure and specificity of the vertebrate anti-mutator uracil-DNA glycosylase SMUG1

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Structure and specificity of the vertebrate anti-mutator uracil-DNA glycosylase SMUG1

Jane E A Wibley et al. Mol Cell. 2003 Jun.
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VSports在线直播 - Abstract

Cytosine deamination is a major promutagenic process, generating G:U mismatches that can cause transition mutations if not repaired. Uracil is also introduced into DNA via nonmutagenic incorporation of dUTP during replication. In bacteria, uracil is excised by uracil-DNA glycosylases (UDG) related to E. coli UNG, and UNG homologs are found in mammals and viruses. Ung knockout mice display no increase in mutation frequency due to a second UDG activity, SMUG1, which is specialized for antimutational uracil excision in mammalian cells VSports手机版. Remarkably, SMUG1 also excises the oxidation-damage product 5-hydroxymethyluracil (HmU), but like UNG is inactive against thymine (5-methyluracil), a chemical substructure of HmU. We have solved the crystal structure of SMUG1 complexed with DNA and base-excision products. This structure indicates a more invasive interaction with dsDNA than observed with other UDGs and reveals an elegant water displacement/replacement mechanism that allows SMUG1 to exclude thymine from its active site while accepting HmU. .

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